Pulmonary herpes simplex virus and cytomegalovirus in patients with acute respiratory distress syndrome related to COVID-19.

Publication date: Jul 17, 2024

Human herpesviruses, particularly cytomegalovirus (CMV) and herpes simplex virus (HSV), frequently reactivate in critically ill patients, including those with acute respiratory distress syndrome (ARDS) related to coronavirus disease 2019 (COVID-19). The clinical interpretation of pulmonary herpesvirus reactivation is challenging and there is ongoing debate about its association with mortality and benefit of antiviral medication. We aimed to quantify the incidence and pathogenicity of pulmonary CMV and HSV reactivations in critically ill COVID-19 patients. Mechanically ventilated COVID-19 patients seropositive for CMV or HSV were included in this observational cohort study. Diagnostic bronchoscopy with bronchoalveolar lavage was performed routinely and analyzed for alveolar viral loads and inflammatory biomarkers. Utilizing joint modeling, we explored the dynamic association between viral load trajectories over time and mortality. We explored alveolar inflammatory biomarker dynamics between reactivated and non-reactivated patients. Pulmonary reactivation (> 10 copies/ml) of CMV occurred in 6% of CMV-seropositive patients (9/156), and pulmonary reactivation of HSV in 37% of HSV-seropositive patients (63/172). HSV viral load dynamics prior to or without antiviral treatment were associated with increased 90-day mortality (hazard ratio [HR] 1. 24, 95% confidence interval [CI] 1. 04-1. 47). The alveolar concentration of several inflammatory biomarkers increased with HSV reactivation, including interleukin (IL)-6, IL-1β, granulocyte colony stimulating factor (G-CSF), and tumor necrosis factor (TNF). In mechanically ventilated COVID-19 patients, HSV reactivations are common, while CMV reactivations were rare. HSV viral load dynamics prior to or without antiviral treatment are associated with mortality. Alveolar inflammation is elevated after HSV reactivation.

Open Access PDF

Concepts Keywords
Biomarkers Antiviral treatment
Herpesviruses Cytomegalovirus (CMV)
Necrosis Viral reactivation
Pulmonary
Routinely

Semantics

Type Source Name
disease MESH herpes simplex
disease MESH acute respiratory distress syndrome
disease MESH COVID-19
disease MESH critically ill
disease VO time
drug DRUGBANK Filgrastim
disease MESH inflammation
disease MESH Bos1
disease MESH infection
disease MESH sepsis
disease MESH lung injury
disease VO Gap
drug DRUGBANK Acyclovir
disease VO population
drug DRUGBANK Dimercaprol
disease VO protocol
disease IDO blood
disease MESH syndrome
drug DRUGBANK Ethylenediamine
drug DRUGBANK Edetic Acid
disease VO manufacturer
drug DRUGBANK Creatinolfosfate
drug DRUGBANK Indoleacetic acid
drug DRUGBANK Ganciclovir
disease VO Viruses
disease IDO assay
disease VO USA
drug DRUGBANK Coenzyme M
disease VO organ
disease IDO process
disease VO age
disease MESH Hypertension
disease MESH Diabetes mellitus
disease MESH COPD
drug DRUGBANK Creatinine
drug DRUGBANK Dexamethasone
drug DRUGBANK Hydrocortisone
disease VO dose
disease MESH hepatitis
disease MESH pulmonary aspergillosis
disease VO volume
drug DRUGBANK Prednisone
drug DRUGBANK Cefotaxime
drug DRUGBANK Tobramycin
drug DRUGBANK Colistin
drug DRUGBANK Nystatin
disease MESH EBV infection
disease MESH aspergillosis
drug DRUGBANK Tocilizumab
disease MESH Pulmonary embolism
disease VO effectiveness
drug DRUGBANK Trestolone
pathway KEGG Viral replication
disease IDO intervention
disease VO frequency
disease MESH viral infections
drug DRUGBANK Ademetionine
disease MESH viremia
disease MESH septic shock
disease MESH Cytomegalovirus infection
disease MESH pneumonia
disease MESH Clinical relevance
disease MESH herpes zoster
disease MESH Fungal infections
drug DRUGBANK Tricyclazole
disease MESH hematologic malignancies
disease MESH reactivation infection
disease MESH influenza

Original Article

(Visited 2 times, 1 visits today)